ORGANIC LETTERS
A Combinatorial Scaffold Approach Based upon a Multicomponent Reaction
2003 Vol. 5, No. 9 1551-1554
Fabio Bertozzi, Birgitte V. Gundersen, Magnus Gustafsson, and Roger Olsson* DiscoVery Chemistry, ACADIA Pharmaceuticals A/S, Fabriksparken 58, DK-2600 Glostrup, Denmark
[email protected] Received February 25, 2003
ABSTRACT
A combinatorial scaffolding procedure for the synthesis and spatial arrangement of tripartite structures was developed.
The design of drug-like chemical entities for nonbiased screening constitutes an enormous challenge.1 Exploring the diversity represented by the amino acid side chains on nonpeptidic scaffolds has proven to be a powerful method for the design of ligands toward a wide range of targets.2 Recently, ligand-based drug design techniques were utilized for identification of novel nonpeptidic ligands at the somatostatin (SST)3 and urotensin II (UII)4 receptors. Both strategies were based on the minimal peptidic motif required (1) Wess, G.; Urmann, M.; Sickenberger, B. Angew. Chem., Int. Ed. 2001, 40, 3341. (2) (a) Nakayama, K.; Kawato, H. C.; Inagaki, H.; Ohta, T. Org. Lett 2001, 3, 3447. (b) Orner, B. P.; Ernst, J. T.; Hamilton, A. D. J. Am. Chem. Soc. 2001, 123, 5382. (c) Hirschmann, R.; Hynes, J., Jr.; Cichy-Knight, M. A.; van Rijn, R. D.; Sprengler, P. A.; Spoors, P. G.; Shakespeare, W. C.; Pientranico-Cole, S.; Barbosa, J.; Liu, J.; Yao, W.; Rohrer, S.; Smith, A. B., III J. Med. Chem. 1998, 41, 1382. (d) Olson, G. L.; Cheung, H.-C.; Chiang, E.; Madison, V. S.; Sepinwall, J.; Vincent, G. P.; Winokur, A.; Gary, K. A. J. Med. Chem. 1995, 38, 2866. (e) Hirschmann, R.; Nicolaou, K. C.; Pietranico, S.; Salvino, J.; Leahy, E. M.; Sprengler, P. A.; Furst, G.; Smith, A. B., III; Strader, C. D.; Cascieri, M. A.; Candelore, M. R.; Donaldson, C.; Vale, W.; Maechler, L. J. Am. Chem. Soc. 1992, 114, 9217. (f) Be´langer, P. C.; Dufresne, C. Can. J. Chem. 1986, 64, 1514. (g) Souers, A. J.; Virgilio, A. A.; Rosenquist, Å.; Fenuik, W.; Ellman, J. A. J. Am. Chem. Soc. 1999, 121, 1817. (3) Rohrer, S. P.; Birzin, E. T.; Mosley, R. T.; Berk, S. C.; Hutchins S. M.; Shen, D.-M.; Xiong, Y.; Hayes, E. C.; Parmar, R. M.; Foor, F.; Mitra, S. W.; Degrado, S. J.; Shu, M.; Klopp, J. M.; Cai, S.-J.; Blake, A.; Chan, W. W. S.; Pasternak, A.; Yang, L.; Patchett, A. A.; Smith, R. G.; Chapman, K. T.; Schaeffer, J. M. Science 1998, 282, 737. (4) Flohr, S.; Kurz, M.; Kostenis, E.; Brkovich, A.; Fournier, A.; Klabunde, T. J. Med. Chem. 2002, 45, 1799. 10.1021/ol0343313 CCC: $25.00 Published on Web 04/05/2003
© 2003 American Chemical Society
for the biological activity, Tyr-D-Trp-Lys and Trp-Lys-Tyr, respectively. Contemporaneously, Hacksell and co-workers published the first nonpeptide UII receptor agonist discovered by screening, using the functional assay technology R-SAT.5 It is notable that the discovered agonist resembles the minimalized UII peptide motif. In addition to peptidomimetic design, the spatial arrangement of three amino acid side chains or analogues thereof has also been successful in proteomimetic design, mimicking the R-helix.2b Overall, these examples signify the importance of the subtle threedimensional arrangement of the three amino acid side chains. This is especially evident in the case of SST and UII ligands, where the same triad of pharmacophore elements results in activity at different receptors. Combinatorial scaffold approaches have mainly been based on the decoration of core structures, e.g. dichloroheterocycles,6 or by formation of the skeleton during the addition of the diversity generating building blocks, i.e., diversityoriented synthesis.7 We herein report a conceptually distinct methodology of combinatorial scaffolding built upon first (5) Croston, G. E.; Olsson, R.; Currier, E. A.; Burstein, E. S.; Weiner, D.; Nash, N.; Severance, D.; Allenmark, S. G.; Thunberg, L.; Ma, J.-N.; Mohell, N.; O’Dowd, B.; Brann, M. R.; Hacksell, U. J. Med. Chem. 2002, 45, 4950. (6) Ding, S.; Gray, N. S.; Wu. X.; Ding, Q.; Shultz, P. G. J. Am. Chem. Soc. 2002, 124, 1594. (7) Kwon, O.; Park, S. B.; Schreiber, S. L. J. Am. Chem. Soc. 2002, 124, 13402.
Scheme 1.
Metal Iodide Promoted Three-Component Reaction
generating the three necessary pharmacophore elements followed by constructing the central core unit as a fourth diversity point. This fourth diversity point is mainly the diverse spatial arrangement of the pharmacophore elements. R,β-Enones have been used as branching points for the creation of drug-like heterocyclic libraries8 and were therefore regarded as useful intermediates to set the stage for the construction of the core structures. However, a drawback was that most of the published synthetic procedures of R,βenones gave only products with two diversity points. With the combinatorial scaffolding objectives in mind, we recently developed a practical and efficient multicomponent reaction (MCR) by which substituted pyrrolidines and R,β-enones incorporating three diversity points could be synthesized (Scheme 1).9 Furthermore, these reactions were applicable toward a diverse range of substrates and the products were easily purified by a scavenger resin/ion exchange chromatography procedure. The chemistry described herein is exemplified by using the structural motif found in the UII10 receptor agonist (AC7954) previously discovered in our laboratories (Scheme 2).5 Mixing cyclopropyl phenyl ketone, 4-chlorobenzaldehyde, and ethylamine in the presence of MgI2 afforded pyrrolidine 1 in 69% yield with an excellent diastereomeric ratio (>99: 1). The central R,β-enone 2 was synthesized in a similar way as pyrrolidine 1, with two exceptions. First, a secondary amine, diethylamine, was used instead of ethylamine and second, to complete a Hofmann elimination of the formed intermediate pyrrolidinium salt, KOtBu was added at room (8) (a) Marzinzik, A. L.; Felder, E. R. J. Org. Chem. 1998, 63, 723. (b) Powers, D. G.; Casebier, D. S.; Fokas, D.; Ryan, W. J.; Troth, J. R.; Coffen, D. L. Tetrahedron 1998, 54, 4085. (9) (a) Bertozzi, F.; Gustafsson, M.; Olsson, R. Org. Lett. 2002, 4, 3147. (b) Bertozzi, F.; Gustafsson, M.; Olsson, R. Org. Lett. 2002, 4, 4333. For similar reaction see: (c) Alper, P. B.; Meyers, C.; Lerchner, A.; Siegel, D. R.; Carreira, E. M. Angew. Chem., Int. Ed. 1999, 38, 3186. Leading MCR references: (d) Biginelli, P. Ber. 1891, 24, 1317. (e) Mannich, C.; Krosche, W. Arch. Pharm. 1912, 250, 647. (f) Passerini, M. Gazz. Chim. Ital. 1921, 51, 126, 181. (g) Ugi, I. Angew. Chem., Int. Ed. Engl. 1962, 1, 8. (h) Do¨mling, A.; Ugi, I. Angew. Chem., Int. Ed. 2000, 39, 3168. (i) Bienayme´, H.; Hulme, C.; Oddon, G.; Schmitt, P. Chem. Eur. J. 2000, 6, 3321. (10) For isolation and structure-function analysis of UII, see: (a) Pearson, D.; Shively, J. E.; Clark, B. R.; Geschwind, I. I.; Barkley, M.; Nishioka, R. S.; Bern, H. A. Proc. Natl. Acad. Sci. U.S.A. 1980, 77, 5021. (b) Coulouarn, Y.; Lihrmann, I.; Jegou, S.; Anouar, Y.; Tostivint, H.; Beauvillian, J. C.; Conlon, J. M.; Bern, H. A.; Vaudry, H. Proc. Natl. Acad. Sci. U.S.A. 1998, 95, 15803. 1552
temperature 2 h prior to the aqueous workup. This procedure gave the R-substituted-R,β-enone 2 in 48% isolated yield with an E/Z ratio of 85:15. Using Et2AlI instead of MgI2 as the Lewis acid afforded 2 in 60% yield without any change in the E/Z ratio. Although R,β-enones have been widely used for the creation of a range of heterocycles, only a few reported examples have incorporated R-substituents and to the best of our knowledge none with additional heteroatom functionalities such as basic amines. The synthesis of five druglike core structures (3-7) was selected to exemplify the use of R-substituted-R,β-enones (e.g. 2) as building blocks. Reaction of N-methylurea with 2 at room temperature in the presence of NaOEt proceeded uneventfully and resulted in dihydropyrimidinone 3 in 48% yield as a single regioisomer. 1H NMR experiments showed two singlets at 6.60 and 4.48 ppm assigned as NH and H6, respectively, corroborating the previously assigned structure.8a Reaction of excess dimethyloxosulfonium methylide with 2 resulted in the formation of cyclopropyl ketone 4 as the major product in 70% isolated yield.11 Only one diastereoisomer was indicated by NMR experiments, and the relative stereochemistry was determined to be anti by NOE measurements. Oxirane byproducts were formed in minor amounts (